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A multicomponent bioactive tissue-engineered blood vessel: Fabrication, mechanical evaluation and biological evaluation with physiological-relevant conditions.

机译:多组分生物活性组织工程血管:具有生理相关条件的制造,机械评估和生物学评估。

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摘要

The high long-term failure rate of synthetic vascular grafts in the replacement of small vessels is known to be associated with the lack of physiological signals to vascular cells causing adverse hemodynamic, inflammatory or coagulatory events. Current studies focus on developing engineered vascular devices with ability of directing cell activity in vitro and in vivo for tissue regeneration. It is also known that controlled molecule release from scaffolds can dramatically increase the scaffold ability of directing cell activities in vitro and in vivo for tissue regeneration. To address the mechanical and biological problems associated with graft materials, we demonstrated a degradable polyester-fibroin composite tubular scaffolds which shows well-integrated nanofibrous structure, endothelial-conducive surface and anisotropic mechanical property, suitable as engineered vascular constructs.;Tissue regeneration needs not only functional biomolecules providing signaling cues to cells and guide tissue remodeling, but also an adequate modality of molecule delivery. In fact, healthy tissue formation requires specific signals at well-defined place and time. To develop scaffolds with multi-modal presentation of biomolecules, we patterned electrospun nanofibers over the thickness of the 3-dimensional scaffolds by programming the deposition of interpenetrating networks of degradable polymers poly(a-caprolactone) and poly(lactide-co-glycolide) acid in tailored proportion. Fluorescent model molecules, drug and growth factors were embedded in the polymeric fibers with different techniques and release profiles were obtained and discussed.;Fabrication process resulted in precise gradient patterns of materials and functional biomolecules throughout the thickness of the scaffold. These graded materials showed programmable spatio-temporal control over the release. Molecule release profiles on each side of the scaffolds were used to determine the separation efficiency of molecule delivery, which achieved >90% for proteins in 200microm scaffolds. Gradient-patterned scaffolds were also used to program simultaneous release of two proteins to the opposite sides of the scaffold and sequential release of proteins to a defined space, which further demonstrate the ability of patterned nanofibers to spatially and temporally confine sustained release. Moreover, results showed that temporal release kinetics could be altered by the structural patterns. Thus, the hierarchically-structured scaffolds presented here may enable development of novel multifunctional scaffolds with defined 3D dynamic microenvironments for tissue regeneration.
机译:已知合成血管移植物在替换小血管中的高长期失败率与缺乏对血管细胞的生理信号有关,从而导致不利的血液动力学,炎症或凝血事件。当前的研究集中在开发具有工程设计的血管装置,该装置具有在体外和体内指导细胞活性进行组织再生的能力。还已知受控的分子从支架释放可以显着增加指导体外和体内细胞活性进行组织再生的支架能力。为了解决与移植材料相关的机械和生物学问题,我们展示了一种可降解的聚酯-纤维蛋白复合管状支架,该支架显示出良好整合的纳米纤维结构,血管内皮表面和各向异性的机械性能,适合用作工程化的血管构建体;不需要组织再生仅功能性生物分子向细胞提供信号提示并指导组织重塑,而且还具有足够的分子递送方式。实际上,健康组织的形成需要在明确定义的位置和时间发出特定信号。为了开发具有生物分子多模态表现的支架,我们通过编程可降解聚合物聚(α-己内酯)和聚(丙交酯-乙交酯)酸互穿网络的沉积,在3维支架的整个厚度上对电纺纳米纤维进行了构图按量身定做。通过不同的技术将荧光模型分子,药物和生长因子嵌入聚合物纤维中,并获得并讨论了释放曲线。制备过程导致了整个支架材料上材料和功能性生物分子的精确梯度模式。这些分级的材料显示了对发布的可编程时空控制。支架两侧的分子释放曲线用于确定分子传递的分离效率,对于200微米支架中的蛋白质,该效率达到了90%以上。梯度模式的支架还用于编程将两种蛋白质同时释放到支架的相对侧,以及将蛋白质顺序释放到限定的空间,这进一步证明了带图案的纳米纤维在空间和时间上限制持续释放的能力。此外,结果表明,暂时释放动力学可以通过结构模式改变。因此,本文介绍的分层结构支架可以使具有定义的3D动态微环境的新型多功能支架能够用于组织再生。

著录项

  • 作者

    Bonani, Walter.;

  • 作者单位

    University of Colorado at Boulder.;

  • 授予单位 University of Colorado at Boulder.;
  • 学科 Engineering Biomedical.;Engineering Materials Science.
  • 学位 Ph.D.
  • 年度 2012
  • 页码 186 p.
  • 总页数 186
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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